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Unique mechanism of target recognition by PfoI restriction endonuclease of the CCGG-family. | LitMetric

AI Article Synopsis

  • Restriction endonucleases (REs) from the CCGG-family recognize specific DNA sequences with variations around a CCGG core and utilize a unique nuclease fold for their function.
  • PfoI, a member of this family, targets a 7 bp sequence and has a distinct active site arrangement that allows it to flip nucleotides but does not compress the DNA like other family members.
  • The study reveals that PfoI alters the DNA backbone conformation significantly to facilitate recognition and cleavage, highlighting the diverse mechanisms used by REs to interact with similar DNA sequences.

Article Abstract

Restriction endonucleases (REs) of the CCGG-family recognize a set of 4-8 bp target sequences that share a common CCGG or CCNGG core and possess PD…D/ExK nuclease fold. REs that interact with 5 bp sequence 5'-CCNGG flip the central N nucleotides and 'compress' the bound DNA to stack the inner base pairs to mimic the CCGG sequence. PfoI belongs to the CCGG-family and cleaves the 7 bp sequence 5'-T|CCNGGA ("|" designates cleavage position). We present here crystal structures of PfoI in free and DNA-bound forms that show unique active site arrangement and mechanism of sequence recognition. Structures and mutagenesis indicate that PfoI features a permuted E…ExD…K active site that differs from the consensus motif characteristic to other family members. Although PfoI also flips the central N nucleotides of the target sequence it does not 'compress' the bound DNA. Instead, PfoI induces a drastic change in DNA backbone conformation that shortens the distance between scissile phosphates to match that in the unperturbed CCGG sequence. Our data demonstrate the diversity and versatility of structural mechanisms employed by restriction enzymes for recognition of related DNA sequences.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6344858PMC
http://dx.doi.org/10.1093/nar/gky1137DOI Listing

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